US20200086314A1 - Chip for sample detection and packaging method thereof - Google Patents

Chip for sample detection and packaging method thereof Download PDF

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Publication number
US20200086314A1
US20200086314A1 US16/691,541 US201916691541A US2020086314A1 US 20200086314 A1 US20200086314 A1 US 20200086314A1 US 201916691541 A US201916691541 A US 201916691541A US 2020086314 A1 US2020086314 A1 US 2020086314A1
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Prior art keywords
covering plate
chip
substrate
face
gap
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US16/691,541
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Zhanhui Wang
Fanglu CHEN
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Suzhou Mnchip Technologies Co Ltd
Tianjin Mnchip Technologies Co Ltd
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Suzhou Mnchip Technologies Co Ltd
Tianjin Mnchip Technologies Co Ltd
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Assigned to TIANJIN MNCHIP TECHNOLOGIES CO., LTD., SUZHOU MNCHIP TECHNOLOGIES CO., LTD. reassignment TIANJIN MNCHIP TECHNOLOGIES CO., LTD. ASSIGNMENT OF ASSIGNORS INTEREST (SEE DOCUMENT FOR DETAILS). Assignors: WANG, ZHANHUI
Assigned to TIANJIN MNCHIP TECHNOLOGIES CO., LTD. reassignment TIANJIN MNCHIP TECHNOLOGIES CO., LTD. EMPLOYMENT AGREEMENT Assignors: CHEN, Fanglu
Publication of US20200086314A1 publication Critical patent/US20200086314A1/en
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    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L3/00Containers or dishes for laboratory use, e.g. laboratory glassware; Droppers
    • B01L3/50Containers for the purpose of retaining a material to be analysed, e.g. test tubes
    • B01L3/502Containers for the purpose of retaining a material to be analysed, e.g. test tubes with fluid transport, e.g. in multi-compartment structures
    • B01L3/5027Containers for the purpose of retaining a material to be analysed, e.g. test tubes with fluid transport, e.g. in multi-compartment structures by integrated microfluidic structures, i.e. dimensions of channels and chambers are such that surface tension forces are important, e.g. lab-on-a-chip
    • B01L3/502707Containers for the purpose of retaining a material to be analysed, e.g. test tubes with fluid transport, e.g. in multi-compartment structures by integrated microfluidic structures, i.e. dimensions of channels and chambers are such that surface tension forces are important, e.g. lab-on-a-chip characterised by the manufacture of the container or its components
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L2200/00Solutions for specific problems relating to chemical or physical laboratory apparatus
    • B01L2200/06Fluid handling related problems
    • B01L2200/0689Sealing
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L2300/00Additional constructional details
    • B01L2300/08Geometry, shape and general structure
    • B01L2300/0803Disc shape
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L2300/00Additional constructional details
    • B01L2300/08Geometry, shape and general structure
    • B01L2300/0887Laminated structure
    • BPERFORMING OPERATIONS; TRANSPORTING
    • B01PHYSICAL OR CHEMICAL PROCESSES OR APPARATUS IN GENERAL
    • B01LCHEMICAL OR PHYSICAL LABORATORY APPARATUS FOR GENERAL USE
    • B01L2300/00Additional constructional details
    • B01L2300/12Specific details about materials

Definitions

  • the present application relates to the field of sample detection technologies, in particular to a chip for sample detection and a packaging method thereof.
  • Microfluidic chip technology is a systematic science technology for precisely controlling a very small amount of fluid (generally microliter, nanoliter or picoliter magnitude) in micron-scale flow channels, and is an important information collection and processing platform for modern biological and chemical science.
  • Application of such a technology can integrate or substantially integrate basic operations used in the biochemical fields, such as sample preparation, reaction, detection, separation or cell culture, sorting, lysis, etc., into a microchip, and a network is formed by micro channels, so that the fluid may be controlled throughout a whole system.
  • This not only enables automated operations, detection and analysis in the traditional biological and chemical experiments, but also successfully implements some experiments that are difficult or impossible to be completed under a traditional biological and chemical mean.
  • the microfluidic chip technology has been widely used in biology, chemistry, medicine and other fields for its advantages of flexible combination and scale integration of various unit technologies on a whole controllable micro platform.
  • embodiments of the present application is dedicated to providing a chip for sample detection and a packaging method thereof to solve the technical problem that when the chip in the prior art is applied in the field of optical detection, production cost of the chip is high because the material itself has high requirements on light transmittance, production process is relatively complex, and the like.
  • One aspect of the present application provides a chip for sample detection, which includes: a substrate; an upper covering plate disposed above the substrate; and a lower covering plate disposed under the substrate. A gap between an upper end face of the substrate and the upper covering plate is sealed, a gap between a lower end face of the substrate and the lower covering plate is sealed, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.
  • the chip is a microfluidic chip
  • the via hole includes one or more of a micro channel, a reaction chamber and a detection chamber.
  • the gap between the upper end face of the substrate and the upper covering plate is directly sealed, and/or the gap between the lower end face of the substrate and the lower covering plate is directly sealed.
  • the gap between the upper end face of the substrate and the upper covering plate is sealed by a medium, and/or the gap between the lower end face of the substrate and the lower covering plate is sealed by a medium.
  • the medium is composed of an adhesive layer.
  • the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
  • the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of one of silicon, glass, and quartz.
  • the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of a thermoplastic polymer.
  • the thermoplastic polymer includes one or more of polydimethyl methacrylate, polycarbonate, polystyrene, polyamide, and polyethylene terephthalate.
  • Another aspect of the present application provides a packaging method of a chip for sample detection, which includes: sealing a gap between an upper end face of a substrate and an upper covering plate; and sealing a gap between a lower end face of the substrate and a lower covering plate.
  • the substrate is disposed between the upper covering plate and the lower covering plate, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.
  • the sealing a gap between an upper end face of a substrate and an upper covering plate includes: binding an adhesive layer and the upper covering plate; and sealing the gap between the upper covering plate which is bound to the adhesive layer and the upper end face of the substrate.
  • the sealing a gap between a lower end face of the substrate and a lower covering plate includes: binding an adhesive layer and the lower covering plate; and sealing the gap between the lower covering plate which is bound to the adhesive layer and the lower end face of the substrate.
  • the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
  • the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of one of glass, quartz and a thermoplastic polymer.
  • the chip is a microfluidic chip
  • the via hole includes one or more of a micro channel, a reaction chamber and a detection chamber.
  • the via hole designed on the substrate of the chip is penetrated, so requirements of a material of the substrate for light transmittance is reduced, so that selection of the material of the substrate is not limited, which on the one hand reduces material cost, and on the other hand, correspondingly reduces processing requirements in production process of the chip to simplify a production process flow.
  • a chip structure proposed in the embodiments adds a covering plate structure which needs to select a material with excellent light transmittance, pure material cost of a material of the upper/lower covering plate is only about 1/10 of cost of the material of the substrate, and there is no structure of the functional channel and the chamber, so manufacturing and processing cost may be correspondingly low. Therefore, the chip structure provided in the embodiments greatly reduces overall cost of the chip while satisfying the light transmittance.
  • the reaction chamber, the detection chamber and/or the functional channel which are penetrating the substrate are sealed together by the upper covering plate and the lower covering plate to form a relatively sealed microfluidic system inside the chip, thereby realizing functions of the chip while meeting the requirements of the chip for the light transmittance, and a packaging procedure is simple and easy to operate.
  • FIG. 1 is a schematic structural diagram of a microfluidic chip in the prior art.
  • FIG. 2 is a schematic structural diagram of a chip for sample detection according to an embodiment of the present application.
  • FIG. 3( a ) is a schematic structural diagram of a chip for sample detection according to another embodiment of the present application.
  • FIG. 3( b ) is a sectional diagram along line A 1 -A 2 shown in FIG. 3( a ) in which the chip for sample detection is shown.
  • FIG. 4 is a flow chart of a packaging method of a chip for sample detection according to an embodiment of the present application.
  • FIG. 5 is a flow chart of a packaging method of a chip for sample detection according to another embodiment of the present application.
  • FIG. 1 is a schematic structural diagram of a microfluidic chip in the prior art.
  • the current microfluidic chip is mainly composed of two parts which includes a substrate 11 and a covering plate 12 , and a micro channel 13 is formed on the substrate 11 , and the substrate 11 having the micro channel 13 is packaged with a covering plate 12 , which makes the micro channel 13 be in a relatively sealed state.
  • the sample to be detected and a reagent are placed in a detection region to do the reaction, and substances generated after the detection and reaction are detected by an optical method.
  • material of the chip has a very small degree of absorption of light to reduce the influence of the material itself on the optical detection as much as possible.
  • the chip has high requirements on light transmittance (especially ultraviolet band light, in 340 nm wavelength), so a material with excellent transmittance is selected as the material of the chip generally, such as plastic, glass or quartz.
  • the price of the material itself is relatively expensive, and a plurality of micro channels and various chambers for the optical detection may be designed on the substrate of the chip, which requires high processing requirements, making production process more complicated and further leading to high production cost of the chip.
  • FIG. 2 is a schematic structural diagram of a chip for sample detection according to an embodiment of the present application.
  • the chip includes a substrate 22 a; an upper covering plate 21 a disposed above the substrate 22 a; and a lower covering plate 23 a disposed under the substrate 22 a.
  • a gap between an upper end face of the substrate 22 a and the upper covering plate 21 a is sealed, a gap between a lower end face of the substrate 22 a and the lower covering plate 23 a is sealed, and the substrate 22 a is provided with a via hole 24 a penetrating the upper end face and the lower end face.
  • a shape and a size of the upper covering plate 21 a and the lower covering plate 23 a are the same as that of the substrate 22 a, and a shape of the chip may be circular, oval, rectangle, square or another arbitrary polygon.
  • a plate generally having a thickness of more than 0.5 mm
  • a film generally having a thickness of less than 0.5 mm
  • the material of the upper covering plate 21 a and the material of the lower covering plate 23 a may be the same or different, and may be specifically selected from a material with good light transmittance, such as glass, quartz or thermoplastic polymers.
  • the processing manners of the upper covering plate 21 a and the lower covering plate 23 a may be the same or different, and may adopt manufacturing process such as injection molding and die-cutting, which is not limited in the present application.
  • the material of the substrate 22 a may be selected from a material with good light transmittance, such as glass, quartz or thermoplastic polymers, or a material such as metal or alloy, as long as the penetrated via hole 24 a may be formed on the substrate 22 a, which is not limited in the present application.
  • the processing manner of the substrate 22 a may be selected from the manners such as injection molding, precision carving or 3D printing, which is also not limited in the present application.
  • a sealing method of the gap between the upper end face of the substrate 22 a and the upper covering plate 21 a and the gap between the lower end face of the substrate 22 a and the lower covering plate 23 a may be the same or different.
  • the sealing method mainly includes two types which includes a direct packaging method and an indirect packaging method.
  • the direct packaging method refers to a method in which contact surfaces of material of the chip reach a molten state by means of heating, ultrasonic vibration, etc., and then two layers of a chip structure will be packaged together by curing, specifically including a heat sealing method, a laser welding method or an ultrasonic welding method, etc., without needs for other medium between the two layers of the chip.
  • the indirect packaging method mainly involves sticking a medium between the two layers and sealing the two layers of the chip structure by curing the medium.
  • the medium in the middle is generally composed of an adhesive layer, which specifically may be made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
  • a gap between the upper end face of the substrate 22 a and the upper covering plate 21 a and a gap between the lower end face of the substrate 22 a and the lower covering plate 23 a are sealed by the direct packaging method.
  • one of the gap between the upper end face of the substrate 22 a and the upper covering plate 21 a and the gap between the lower end face of the substrate 22 a and the lower covering plate 23 a may also be selected to adopt the indirect packaging method, the other adopts the direct packaging method, or both adopt the indirect packaging method.
  • the via hole 24 a specifically includes a reaction chamber, a detection chamber, and/or a functional channel configured to connect the reaction chamber and the detection chamber, and the like.
  • a shape and number of the via holes 24 a may be differently set according to specific demands or actual demands, for example, the shape of the via holes 24 a may be selected from a circle, an ellipse, a square or other polygons, and the number of the via holes 24 a may be 1 to 30 or more than 30, and the shape and the number of the via holes 24 a are not limited in the present application.
  • a distribution position of the via holes 24 a on the substrate 22 a is also set according to the actual demands of those skilled in the art, and is generally distributed outwardly at a center of the chip.
  • the via hole designed on the substrate of the chip is penetrated, so requirements of a material of the substrate for light transmittance is reduced, so that selection of the material of the substrate is not limited, which on the one hand reduces material cost, and on the other hand, correspondingly reduces processing requirements in production process of the chip to simplify a production process flow.
  • a chip structure proposed in the embodiments adds a covering plate structure which needs to select a material with excellent light transmittance, since pure material cost of a material of the upper/lower covering plate is only about 1/10 of cost of the material of the substrate, and there is no structure of the functional channel and the chamber, manufacturing and processing cost may be correspondingly low. Therefore, the chip structure provided in the embodiments greatly reduces overall cost of the chip while satisfying the light transmittance.
  • FIG. 3( a ) is a schematic structural diagram of a chip for sample detection according to another embodiment of the present application.
  • the embodiment is basically the same as the embodiment shown in FIG. 2 , and the differences will be mainly described below, and the same portions will not be repeatedly described.
  • the chip for sample detection provided in the embodiment is a microfluidic chip, and includes a substrate 22 b, an upper covering plate 21 b disposed above the substrate 22 b, and a lower covering plate 23 b disposed under the substrate 22 b.
  • the substrate 22 b is provided with a detection chamber, a reaction chamber 25 and a micro channel 26 , the detection chamber is penetrating, and the reaction chamber 25 and the micro channel 26 are non-penetrating, i.e., via holes 24 b only include the detection chamber.
  • the microfluidic chip is configured to detect an index in the human body. As long as the detection chamber has high light transmittance, the reaction chamber 25 and the micro channel 26 have no special requirements for the light transmittance, so the reaction chamber 25 and the micro channel 26 can be set to be non-penetrating.
  • one or more of the reaction chamber, the detection chamber and the micro channel may be designed as a form of the via hole according to specific demands, which is not limited in the present application.
  • the reaction chamber 25 and the micro channel 26 are disposed in an intermediate region of the chip, and the detection chamber (i.e., the via holes 24 b ) is disposed at an edge of the chip around the reaction chamber 25 and the micro channel 26 .
  • the detection chamber i.e., the via holes 24 b
  • the detection chambers and the micro channels 26 may also be differently set according to the specific demands of those skilled in the art, which are not specifically limited in the present application.
  • a size and a shape of a plurality of via holes 24 b on a same chip may be the same or different, and those skilled in the art may also make different selections according to the specific demands, which is not limited in the present application.
  • the upper covering plate 21 b and/or the lower covering plate 23 b in the embodiment are made of a material of a transparent film, and a thickness of the transparent film is generally from 0.05 mm to 0.5 mm.
  • the material may be selected from thermoplastic polymers, specifically including one or more of PMMA (polymethyl methacrylate), PC (polycarbonate), PS (polystyrene), PA (polyamide) and PET (polyethylene terephthalate).
  • PMMA polymethyl methacrylate
  • PC polycarbonate
  • PS polystyrene
  • PA polyamide
  • PET polyethylene terephthalate
  • the substrate 22 b may be made of ABS resin (acrylonitrile butadiene styrene copolymer) or PMMA, which has characteristics of high strength, good toughness, low cost, easy processing and molding.
  • ABS resin acrylonitrile butadiene styrene copolymer
  • PMMA polymethyl methacrylate
  • the gap between the upper end face of the substrate 22 b and the upper covering plate 21 b and the gap between the lower end face of the substrate 22 b and the lower covering plate 23 b are sealed by the indirect packaging method.
  • upper and lower layers of the chip structure are sealed together by curing an adhesive layer, and the adhesive layer is specifically made of one of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive and an optical grade double-sided adhesive.
  • the chip for sample detection provided by the embodiments is substantially the microfluidic chip, and the reaction chamber, the detection chamber and the penetrated micro channel on the substrate are packaged together by the upper covering plate and the lower covering plate to form a relatively sealed microfluidic system inside the chip, which realizes functions of the microfluidic chip and reduces the requirements of the material of the substrate for ultraviolet band light transmittance.
  • the material of the upper covering plate and/or the lower covering plate are made of the thermoplastic polymer, which have lower cost and manufacturing and processing cost and are suitable for large-scale industrial production.
  • the indirect packaging method adopted between the substrate and the upper covering plate and between the substrate and the lower covering plate may be performed at normal temperature and does not require specialized equipment for packaging, which improves package yield of the chip and reduces the cost of the chip, and is also suitable for the large-scale industrial production.
  • the light transmittance of the specific chip structure provided in the embodiments will be compared with the light transmittance of a chip structure in the prior art, which will help to understand the present application.
  • specific materials and packaging methods used below are not limited in the present application.
  • the experimental instrument used in the experiment is the Celecare M1, which is an automatic biochemical analyzer (detection wavelength is 340 nm/800 nm) produced by Tianjin MNCHIP Technologies Co., Ltd.
  • the instrument mainly detects the light transmittance of the chip for 340 nm ultraviolet band light.
  • the chips to be detected were divided into two groups.
  • the first group is the chip structure in the embodiment of the present application, including upper and lower covering plates, and a detection hole in the substrate is penetrated.
  • the material of the substrate is high transmittance PMMA, and the materials of the upper covering plate and the lower covering plate are respectively adopted a PC film with high light transmittance, and a gap between the upper covering plate and the substrate and a gap between the lower covering plate and the substrate are respectively sealed by the pressure-sensitive double-sided adhesive.
  • the second group is the chip structure in the prior art, which only includes the upper covering plate, and the detection hole in the substrate is not penetrated.
  • the material of the substrate is the PMMA with high light transmittance
  • the upper covering plate is made of the PC film with high light transmittance
  • a gap between the upper covering plate and the substrate is sealed by the pressure-sensitive double-sided adhesive.
  • the two groups of chips were respectively performed light source exposure detection and light intensity values before and after the light passed through the upper covering plate of the PC film were counted, thus the absorbance degrees and transmittance were calculated.
  • Each group includes 10 pieces of test samples, and test result is shown in Table 1.
  • the light transmittance of the second group of chip i.e. the chip in the prior art
  • that of the first group of chip i.e. the chip in the embodiment of the present application
  • the chip structure provided in the embodiment of the present application reduces the overall cost and simplifies the production process under a condition of improving the light transmittance of the chip itself.
  • FIG. 4 is a flow chart of a method for packaging a chip for sample detection according to an embodiment of the present application. As shown in FIG. 4 , the method includes:
  • Step 401 sealing a gap between an upper end face of a substrate and an upper covering plate
  • Step 402 sealing a gap between a lower end face of the substrate and a lower covering plate; the substrate being disposed between the upper covering plate and the lower covering plate, and the substrate being provided with a via hole penetrating the upper end face and the lower end face.
  • a shape and a size of the upper covering plate/lower covering plate described above are the same as that of the substrate, which may be either a plate (generally having a thickness of more than 0.5 mm) or a film material (generally having a thickness of less than 0.5 mm).
  • the material of the upper covering plate and the lower covering plate may be the same or different, and are specifically replaced by a material with better light transmittance, such as glass, quartz or thermoplastic polymers.
  • the processing manners of the upper covering plate and the lower covering plate may adopt manufacturing process such as injection molding and die-cutting, and the like.
  • the material of the substrate is not limited, which may be selected from a material with good light transmittance, such as glass, quartz or thermoplastic polymers, and a material such as a metal or an alloy, as long as the penetrated via hole can be formed on the substrate.
  • the processing manner of the substrate may be selected from the manners such as the injection molding, carving or 3D printing.
  • the via hole specifically includes a reaction chamber, a detection chamber, and/or a functional channel configured to connect the reaction chamber and the detection chamber, and the like.
  • a shape and number of the via holes may be differently set according to specific demands or actual demands, for example, the shape of the via holes may be selected from a circle, an ellipse, a square or other polygons, and the number of the via holes may be 1 to 30 or more than 30.
  • a distribution position of the via holes on the substrate may also be set according to the actual demands of those skilled in the art before preparing to process the substrate.
  • the reaction chamber, the detection chamber and/or the functional channel which are penetrating the substrate are sealed together by the upper covering plate and the lower covering plate to form a relatively sealed microfluidic system inside the chip, thereby realizing functions of the chip while meeting the requirements of the chip for the light transmittance, and a packaging procedure is simple and easy to operate.
  • FIG. 5 is a flow chart of a method for packaging a chip for sample detection according to another embodiment of the present application.
  • the packaging method provided in the embodiment of the present application includes:
  • Step 501 binding an adhesive layer and the upper covering plate
  • Step 502 sealing the gap between the upper covering plate which is bound to the adhesive layer and the upper end face of the substrate;
  • Step 503 binding an adhesive layer and the lower covering plate
  • Step 504 sealing the gap between the lower covering plate which is bound to the adhesive layer and the lower end face of the substrate; the substrate being disposed between the upper covering plate and the lower covering plate, and the substrate being provided with a via hole penetrating the upper end face and the lower end face.
  • the via hole described above includes one or more of a reaction chamber configured to perform various biochemical reactions, a detection chamber configured to perform biochemical detection and a micro channel configured to form connecting channels.
  • the number and the shape of the via holes may be differently set according to demands, and the chip formed may be a microfluidic chip.
  • the material of the upper covering plate and/or the lower covering plate may be adopted thermoplastic polymers, specifically including one or more of PMMA (polymethyl methacrylate), PC (polycarbonate), PS (polystyrene), PA (polyamide) and PET (polyethylene terephthalate).
  • thermoplastic polymers specifically including one or more of PMMA (polymethyl methacrylate), PC (polycarbonate), PS (polystyrene), PA (polyamide) and PET (polyethylene terephthalate).
  • PMMA polymethyl methacrylate
  • PC polycarbonate
  • PS polystyrene
  • PA polyamide
  • PET polyethylene terephthalate
  • the adhesive layer in the middle may be made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive
  • the gap between the upper covering plate and the substrate provided with the penetrated via hole and the gap between the lower covering plate and the substrate provided with the penetrated via hole are respectively sealed by the adhesive layer to form a relatively sealed microfluidic system inside the chip, thereby realizing functions of the microfluidic chip while meeting the requirements of the microfluidic chip for ultraviolet band light transmittance.
  • a packaging process of the microfluidic chip may be performed at normal temperature and does not require specialized equipment for packaging, which improves package yield of the chip and reduces the cost of the chip, and is suitable for large-scale industrial production.

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Abstract

A chip for sample detection includes a substrate, an upper covering plate disposed above the substrate and a lower covering plate disposed under the substrate. A gap between an upper end face of the substrate and the upper covering plate is sealed, a gap between a lower end face of the substrate and the lower covering plate is sealed, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.

Description

    CROSS-REFERENCE TO RELATED APPLICATIONS
  • This application is a continuation of International Application No. PCT/CN2018/086363 filed on May 10, 2018, which claims priority to Chinese patent application No. 201710364719.7 filed on May 22, 2017. Both applications are incorporated herein by reference in their entireties.
    • TECHNICAL FIELD
  • The present application relates to the field of sample detection technologies, in particular to a chip for sample detection and a packaging method thereof.
    • BACKGROUND
  • Microfluidic chip technology is a systematic science technology for precisely controlling a very small amount of fluid (generally microliter, nanoliter or picoliter magnitude) in micron-scale flow channels, and is an important information collection and processing platform for modern biological and chemical science. Application of such a technology can integrate or substantially integrate basic operations used in the biochemical fields, such as sample preparation, reaction, detection, separation or cell culture, sorting, lysis, etc., into a microchip, and a network is formed by micro channels, so that the fluid may be controlled throughout a whole system. This not only enables automated operations, detection and analysis in the traditional biological and chemical experiments, but also successfully implements some experiments that are difficult or impossible to be completed under a traditional biological and chemical mean. The microfluidic chip technology has been widely used in biology, chemistry, medicine and other fields for its advantages of flexible combination and scale integration of various unit technologies on a whole controllable micro platform.
    • SUMMARY
  • In view of this, embodiments of the present application is dedicated to providing a chip for sample detection and a packaging method thereof to solve the technical problem that when the chip in the prior art is applied in the field of optical detection, production cost of the chip is high because the material itself has high requirements on light transmittance, production process is relatively complex, and the like.
  • One aspect of the present application provides a chip for sample detection, which includes: a substrate; an upper covering plate disposed above the substrate; and a lower covering plate disposed under the substrate. A gap between an upper end face of the substrate and the upper covering plate is sealed, a gap between a lower end face of the substrate and the lower covering plate is sealed, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.
  • In one embodiment, the chip is a microfluidic chip, and the via hole includes one or more of a micro channel, a reaction chamber and a detection chamber.
  • In one embodiment, the gap between the upper end face of the substrate and the upper covering plate is directly sealed, and/or the gap between the lower end face of the substrate and the lower covering plate is directly sealed.
  • In one embodiment, the gap between the upper end face of the substrate and the upper covering plate is sealed by a medium, and/or the gap between the lower end face of the substrate and the lower covering plate is sealed by a medium.
  • In one embodiment, the medium is composed of an adhesive layer.
  • In one embodiment, the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
  • In one embodiment, the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of one of silicon, glass, and quartz.
  • In one embodiment, the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of a thermoplastic polymer.
  • In one embodiment, the thermoplastic polymer includes one or more of polydimethyl methacrylate, polycarbonate, polystyrene, polyamide, and polyethylene terephthalate.
  • Another aspect of the present application provides a packaging method of a chip for sample detection, which includes: sealing a gap between an upper end face of a substrate and an upper covering plate; and sealing a gap between a lower end face of the substrate and a lower covering plate. The substrate is disposed between the upper covering plate and the lower covering plate, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.
  • In one embodiment, the sealing a gap between an upper end face of a substrate and an upper covering plate includes: binding an adhesive layer and the upper covering plate; and sealing the gap between the upper covering plate which is bound to the adhesive layer and the upper end face of the substrate.
  • In one embodiment, the sealing a gap between a lower end face of the substrate and a lower covering plate includes: binding an adhesive layer and the lower covering plate; and sealing the gap between the lower covering plate which is bound to the adhesive layer and the lower end face of the substrate.
  • In one embodiment, the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
  • In one embodiment, the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of one of glass, quartz and a thermoplastic polymer.
  • In one embodiment, the chip is a microfluidic chip, and the via hole includes one or more of a micro channel, a reaction chamber and a detection chamber.
  • In the chip for sample detection provided by the embodiments of the present application, the via hole designed on the substrate of the chip is penetrated, so requirements of a material of the substrate for light transmittance is reduced, so that selection of the material of the substrate is not limited, which on the one hand reduces material cost, and on the other hand, correspondingly reduces processing requirements in production process of the chip to simplify a production process flow. Although a chip structure proposed in the embodiments adds a covering plate structure which needs to select a material with excellent light transmittance, pure material cost of a material of the upper/lower covering plate is only about 1/10 of cost of the material of the substrate, and there is no structure of the functional channel and the chamber, so manufacturing and processing cost may be correspondingly low. Therefore, the chip structure provided in the embodiments greatly reduces overall cost of the chip while satisfying the light transmittance.
  • By using the method for packaging the chip for sample detection provided by the embodiments of the present application, the reaction chamber, the detection chamber and/or the functional channel which are penetrating the substrate are sealed together by the upper covering plate and the lower covering plate to form a relatively sealed microfluidic system inside the chip, thereby realizing functions of the chip while meeting the requirements of the chip for the light transmittance, and a packaging procedure is simple and easy to operate.
    • BRIEF DESCRIPTION OF DRAWINGS
  • FIG. 1 is a schematic structural diagram of a microfluidic chip in the prior art.
  • FIG. 2 is a schematic structural diagram of a chip for sample detection according to an embodiment of the present application.
  • FIG. 3(a) is a schematic structural diagram of a chip for sample detection according to another embodiment of the present application.
  • FIG. 3(b) is a sectional diagram along line A1-A2 shown in FIG. 3(a) in which the chip for sample detection is shown.
  • FIG. 4 is a flow chart of a packaging method of a chip for sample detection according to an embodiment of the present application.
  • FIG. 5 is a flow chart of a packaging method of a chip for sample detection according to another embodiment of the present application.
    •  DETAILED DESCRIPTION OF THE EMBODIMENTS
  • In order to make the objects, technical solutions and advantages of the present application clearer, the present application will be further described in detail below in combination with the accompanying drawings.
  • FIG. 1 is a schematic structural diagram of a microfluidic chip in the prior art. As shown in FIG. 1, the current microfluidic chip is mainly composed of two parts which includes a substrate 11 and a covering plate 12, and a micro channel 13 is formed on the substrate 11, and the substrate 11 having the micro channel 13 is packaged with a covering plate 12, which makes the micro channel 13 be in a relatively sealed state.
  • When the microfluidic chip is applied in optical detection, the sample to be detected and a reagent are placed in a detection region to do the reaction, and substances generated after the detection and reaction are detected by an optical method. This requires that material of the chip has a very small degree of absorption of light to reduce the influence of the material itself on the optical detection as much as possible. The chip has high requirements on light transmittance (especially ultraviolet band light, in 340 nm wavelength), so a material with excellent transmittance is selected as the material of the chip generally, such as plastic, glass or quartz. The price of the material itself is relatively expensive, and a plurality of micro channels and various chambers for the optical detection may be designed on the substrate of the chip, which requires high processing requirements, making production process more complicated and further leading to high production cost of the chip.
  • FIG. 2 is a schematic structural diagram of a chip for sample detection according to an embodiment of the present application. As shown in FIG. 2, the chip includes a substrate 22 a; an upper covering plate 21 a disposed above the substrate 22 a; and a lower covering plate 23 a disposed under the substrate 22 a. A gap between an upper end face of the substrate 22 a and the upper covering plate 21 a is sealed, a gap between a lower end face of the substrate 22 a and the lower covering plate 23 a is sealed, and the substrate 22 a is provided with a via hole 24 a penetrating the upper end face and the lower end face.
  • A shape and a size of the upper covering plate 21 a and the lower covering plate 23 a are the same as that of the substrate 22 a, and a shape of the chip may be circular, oval, rectangle, square or another arbitrary polygon.
  • As for the material of the upper covering plate 21 a and the lower covering plate 23 a, a plate (generally having a thickness of more than 0.5 mm) or a film (generally having a thickness of less than 0.5 mm) can be selected. The material of the upper covering plate 21 a and the material of the lower covering plate 23 a may be the same or different, and may be specifically selected from a material with good light transmittance, such as glass, quartz or thermoplastic polymers. Similarly, the processing manners of the upper covering plate 21 a and the lower covering plate 23 a may be the same or different, and may adopt manufacturing process such as injection molding and die-cutting, which is not limited in the present application.
  • The material of the substrate 22 a may be selected from a material with good light transmittance, such as glass, quartz or thermoplastic polymers, or a material such as metal or alloy, as long as the penetrated via hole 24 a may be formed on the substrate 22 a, which is not limited in the present application. The processing manner of the substrate 22 a may be selected from the manners such as injection molding, precision carving or 3D printing, which is also not limited in the present application.
  • A sealing method of the gap between the upper end face of the substrate 22 a and the upper covering plate 21 a and the gap between the lower end face of the substrate 22 a and the lower covering plate 23 a may be the same or different. The sealing method mainly includes two types which includes a direct packaging method and an indirect packaging method. The direct packaging method refers to a method in which contact surfaces of material of the chip reach a molten state by means of heating, ultrasonic vibration, etc., and then two layers of a chip structure will be packaged together by curing, specifically including a heat sealing method, a laser welding method or an ultrasonic welding method, etc., without needs for other medium between the two layers of the chip. The indirect packaging method mainly involves sticking a medium between the two layers and sealing the two layers of the chip structure by curing the medium. The medium in the middle is generally composed of an adhesive layer, which specifically may be made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
  • In the embodiment, as shown in FIG. 2, a gap between the upper end face of the substrate 22 a and the upper covering plate 21 a and a gap between the lower end face of the substrate 22 a and the lower covering plate 23 a are sealed by the direct packaging method. In other embodiments, one of the gap between the upper end face of the substrate 22 a and the upper covering plate 21 a and the gap between the lower end face of the substrate 22 a and the lower covering plate 23 a may also be selected to adopt the indirect packaging method, the other adopts the direct packaging method, or both adopt the indirect packaging method.
  • The via hole 24 a specifically includes a reaction chamber, a detection chamber, and/or a functional channel configured to connect the reaction chamber and the detection chamber, and the like. A shape and number of the via holes 24 a may be differently set according to specific demands or actual demands, for example, the shape of the via holes 24 a may be selected from a circle, an ellipse, a square or other polygons, and the number of the via holes 24 a may be 1 to 30 or more than 30, and the shape and the number of the via holes 24 a are not limited in the present application. A distribution position of the via holes 24 a on the substrate 22 a is also set according to the actual demands of those skilled in the art, and is generally distributed outwardly at a center of the chip.
  • In the chip for sample detection provided in the embodiments, the via hole designed on the substrate of the chip is penetrated, so requirements of a material of the substrate for light transmittance is reduced, so that selection of the material of the substrate is not limited, which on the one hand reduces material cost, and on the other hand, correspondingly reduces processing requirements in production process of the chip to simplify a production process flow. Although a chip structure proposed in the embodiments adds a covering plate structure which needs to select a material with excellent light transmittance, since pure material cost of a material of the upper/lower covering plate is only about 1/10 of cost of the material of the substrate, and there is no structure of the functional channel and the chamber, manufacturing and processing cost may be correspondingly low. Therefore, the chip structure provided in the embodiments greatly reduces overall cost of the chip while satisfying the light transmittance.
  • FIG. 3(a) is a schematic structural diagram of a chip for sample detection according to another embodiment of the present application. The embodiment is basically the same as the embodiment shown in FIG. 2, and the differences will be mainly described below, and the same portions will not be repeatedly described. As shown in FIG. 3(a) and FIG. 3(b), the chip for sample detection provided in the embodiment is a microfluidic chip, and includes a substrate 22 b, an upper covering plate 21 b disposed above the substrate 22 b, and a lower covering plate 23 b disposed under the substrate 22 b. The substrate 22 b is provided with a detection chamber, a reaction chamber 25 and a micro channel 26, the detection chamber is penetrating, and the reaction chamber 25 and the micro channel 26 are non-penetrating, i.e., via holes 24 b only include the detection chamber. The microfluidic chip is configured to detect an index in the human body. As long as the detection chamber has high light transmittance, the reaction chamber 25 and the micro channel 26 have no special requirements for the light transmittance, so the reaction chamber 25 and the micro channel 26 can be set to be non-penetrating. In the microfluidic chip of other embodiments, one or more of the reaction chamber, the detection chamber and the micro channel may be designed as a form of the via hole according to specific demands, which is not limited in the present application.
  • As shown in FIG. 3(a), the reaction chamber 25 and the micro channel 26 are disposed in an intermediate region of the chip, and the detection chamber (i.e., the via holes 24 b) is disposed at an edge of the chip around the reaction chamber 25 and the micro channel 26. In fact, there is no fixed relationship between positions of the reaction chamber 25, the detection chamber and the micro channel 26 and numbers of the reaction chambers 25, the detection chambers and the micro channels 26 may also be differently set according to the specific demands of those skilled in the art, which are not specifically limited in the present application. In addition, a size and a shape of a plurality of via holes 24 b on a same chip may be the same or different, and those skilled in the art may also make different selections according to the specific demands, which is not limited in the present application.
  • The upper covering plate 21 b and/or the lower covering plate 23 b in the embodiment are made of a material of a transparent film, and a thickness of the transparent film is generally from 0.05 mm to 0.5 mm. The material may be selected from thermoplastic polymers, specifically including one or more of PMMA (polymethyl methacrylate), PC (polycarbonate), PS (polystyrene), PA (polyamide) and PET (polyethylene terephthalate). Compared with conventional glass and quartz, the thermoplastic polymers have lower cost and lower manufacturing and processing cost, and are more suitable for large-scale industrial production.
  • The substrate 22 b may be made of ABS resin (acrylonitrile butadiene styrene copolymer) or PMMA, which has characteristics of high strength, good toughness, low cost, easy processing and molding.
  • The gap between the upper end face of the substrate 22 b and the upper covering plate 21 b and the gap between the lower end face of the substrate 22 b and the lower covering plate 23 b are sealed by the indirect packaging method. Specifically, upper and lower layers of the chip structure are sealed together by curing an adhesive layer, and the adhesive layer is specifically made of one of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive and an optical grade double-sided adhesive.
  • The chip for sample detection provided by the embodiments is substantially the microfluidic chip, and the reaction chamber, the detection chamber and the penetrated micro channel on the substrate are packaged together by the upper covering plate and the lower covering plate to form a relatively sealed microfluidic system inside the chip, which realizes functions of the microfluidic chip and reduces the requirements of the material of the substrate for ultraviolet band light transmittance. In addition, the material of the upper covering plate and/or the lower covering plate are made of the thermoplastic polymer, which have lower cost and manufacturing and processing cost and are suitable for large-scale industrial production. The indirect packaging method adopted between the substrate and the upper covering plate and between the substrate and the lower covering plate may be performed at normal temperature and does not require specialized equipment for packaging, which improves package yield of the chip and reduces the cost of the chip, and is also suitable for the large-scale industrial production.
  • Hereinafter, the light transmittance of the specific chip structure provided in the embodiments will be compared with the light transmittance of a chip structure in the prior art, which will help to understand the present application. However, it should be understood that specific materials and packaging methods used below are not limited in the present application.
  • An experimental instrument used in the experiment is the Celecare M1, which is an automatic biochemical analyzer (detection wavelength is 340 nm/800 nm) produced by Tianjin MNCHIP Technologies Co., Ltd. In this experiment, the instrument mainly detects the light transmittance of the chip for 340 nm ultraviolet band light. The chips to be detected were divided into two groups. The first group is the chip structure in the embodiment of the present application, including upper and lower covering plates, and a detection hole in the substrate is penetrated. The material of the substrate is high transmittance PMMA, and the materials of the upper covering plate and the lower covering plate are respectively adopted a PC film with high light transmittance, and a gap between the upper covering plate and the substrate and a gap between the lower covering plate and the substrate are respectively sealed by the pressure-sensitive double-sided adhesive. The second group is the chip structure in the prior art, which only includes the upper covering plate, and the detection hole in the substrate is not penetrated. The material of the substrate is the PMMA with high light transmittance, the upper covering plate is made of the PC film with high light transmittance, and a gap between the upper covering plate and the substrate is sealed by the pressure-sensitive double-sided adhesive.
  • The two groups of chips were respectively performed light source exposure detection and light intensity values before and after the light passed through the upper covering plate of the PC film were counted, thus the absorbance degrees and transmittance were calculated. Each group includes 10 pieces of test samples, and test result is shown in Table 1.
  • TABLE 1
    Data Comparison of Transmittance Experiments
    First group Second group
    Incident Exit Incident Exit
    light light Absorbance light light Absorbance
    intensity intensity degree A0 Transmittance T intensity I0 intensity degree A0 Transmittance T
    I0 (cd) I (cd) (lg(I0/I)) (%) (cd) I (cd) (lg(I0/I)) (%)
    13295 12214 0.03683 0.91869 13321 11210 0.07493 0.84152
    13256 12196 0.03619 0.92003 13305 11232 0.07355 0.84419
    13279 12179 0.03755 0.91716 13352 11225 0.07535 0.84069
    13263 12183 0.03688 0.91857 13296 11165 0.07586 0.83972
    13302 12210 0.03727 0.91790 13315 11245 0.07338 0.84453
    13285 12178 0.03778 0.91667 13288 11196 0.07439 0.84256
    13312 12215 0.03734 0.91759 13321 11221 0.07450 0.84235
    13289 12185 0.03766 0.91692 13279 11187 0.07445 0.84245
    13311 12121 0.03745 0.91736 13310 11206 0.07472 0.84192
    13298 12198 0.03749 0.91728 13321 11210 0.07493 0.84152
  • Through the above comparison experiments, it is found that the light transmittance of the second group of chip (i.e. the chip in the prior art) is only about 84% in the 340 nm band, while that of the first group of chip (i.e. the chip in the embodiment of the present application) is over 91% in the 340 nm band, which fully meets requirements of the chip for the ultraviolet band light transmittance. It can be seen that the chip structure provided in the embodiment of the present application reduces the overall cost and simplifies the production process under a condition of improving the light transmittance of the chip itself.
  • FIG. 4 is a flow chart of a method for packaging a chip for sample detection according to an embodiment of the present application. As shown in FIG. 4, the method includes:
  • Step 401: sealing a gap between an upper end face of a substrate and an upper covering plate;
  • Step 402: sealing a gap between a lower end face of the substrate and a lower covering plate; the substrate being disposed between the upper covering plate and the lower covering plate, and the substrate being provided with a via hole penetrating the upper end face and the lower end face.
  • A shape and a size of the upper covering plate/lower covering plate described above are the same as that of the substrate, which may be either a plate (generally having a thickness of more than 0.5 mm) or a film material (generally having a thickness of less than 0.5 mm). The material of the upper covering plate and the lower covering plate may be the same or different, and are specifically replaced by a material with better light transmittance, such as glass, quartz or thermoplastic polymers. The processing manners of the upper covering plate and the lower covering plate may adopt manufacturing process such as injection molding and die-cutting, and the like.
  • The material of the substrate is not limited, which may be selected from a material with good light transmittance, such as glass, quartz or thermoplastic polymers, and a material such as a metal or an alloy, as long as the penetrated via hole can be formed on the substrate. The processing manner of the substrate may be selected from the manners such as the injection molding, carving or 3D printing.
  • The via hole specifically includes a reaction chamber, a detection chamber, and/or a functional channel configured to connect the reaction chamber and the detection chamber, and the like. A shape and number of the via holes may be differently set according to specific demands or actual demands, for example, the shape of the via holes may be selected from a circle, an ellipse, a square or other polygons, and the number of the via holes may be 1 to 30 or more than 30. A distribution position of the via holes on the substrate may also be set according to the actual demands of those skilled in the art before preparing to process the substrate.
  • By using the method for packaging the chip for sample detection provided by the embodiments of the present application, the reaction chamber, the detection chamber and/or the functional channel which are penetrating the substrate are sealed together by the upper covering plate and the lower covering plate to form a relatively sealed microfluidic system inside the chip, thereby realizing functions of the chip while meeting the requirements of the chip for the light transmittance, and a packaging procedure is simple and easy to operate.
  • FIG. 5 is a flow chart of a method for packaging a chip for sample detection according to another embodiment of the present application. As shown in FIG. 5, the packaging method provided in the embodiment of the present application includes:
  • Step 501: binding an adhesive layer and the upper covering plate;
  • Step 502: sealing the gap between the upper covering plate which is bound to the adhesive layer and the upper end face of the substrate;
  • Step 503: binding an adhesive layer and the lower covering plate;
  • Step 504: sealing the gap between the lower covering plate which is bound to the adhesive layer and the lower end face of the substrate; the substrate being disposed between the upper covering plate and the lower covering plate, and the substrate being provided with a via hole penetrating the upper end face and the lower end face.
  • The via hole described above includes one or more of a reaction chamber configured to perform various biochemical reactions, a detection chamber configured to perform biochemical detection and a micro channel configured to form connecting channels. The number and the shape of the via holes may be differently set according to demands, and the chip formed may be a microfluidic chip.
  • The material of the upper covering plate and/or the lower covering plate may be adopted thermoplastic polymers, specifically including one or more of PMMA (polymethyl methacrylate), PC (polycarbonate), PS (polystyrene), PA (polyamide) and PET (polyethylene terephthalate). Compared with conventional glass and quartz, the thermoplastic polymers have lower cost and lower manufacturing and processing cost, and are more suitable for large-scale industrial production.
  • The adhesive layer in the middle may be made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive
  • By using the method for packaging the chip for sample detection provided by the embodiment, the gap between the upper covering plate and the substrate provided with the penetrated via hole and the gap between the lower covering plate and the substrate provided with the penetrated via hole are respectively sealed by the adhesive layer to form a relatively sealed microfluidic system inside the chip, thereby realizing functions of the microfluidic chip while meeting the requirements of the microfluidic chip for ultraviolet band light transmittance. A packaging process of the microfluidic chip may be performed at normal temperature and does not require specialized equipment for packaging, which improves package yield of the chip and reduces the cost of the chip, and is suitable for large-scale industrial production.
  • The above is only a preferred embodiment of the present application and is not used to limit the protection scope of the present application. Any modifications, equivalent replacement, improvement, etc. made in the spirit and principles of the present application shall be included in the protection scope of the present application.

Claims (20)

What is claimed is:
1. A chip for sample detection, comprising:
a substrate;
an upper covering plate disposed above the substrate; and
a lower covering plate disposed under the substrate,
wherein a gap between an upper end face of the substrate and the upper covering plate is sealed, a gap between a lower end face of the substrate and the lower covering plate is sealed, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.
2. The chip for sample detection of claim 1, wherein the chip is a microfluidic chip, and the via hole comprises one or more of a micro channel, a reaction chamber and a detection chamber.
3. The chip for sample detection of claim 1, wherein the gap between the upper end face of the substrate and the upper covering plate is directly sealed, and/or the gap between the lower end face of the substrate and the lower covering plate is directly sealed.
4. The chip for sample detection of claim 1, wherein the gap between the upper end face of the substrate and the upper covering plate is sealed by a medium, and/or the gap between the lower end face of the substrate and the lower covering plate is sealed by a medium.
5. The chip for sample detection of claim 4, wherein the medium is composed of an adhesive layer.
6. The chip for sample detection of claim 5, wherein the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
7. The chip for sample detection of claim 1, wherein the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of one of glass and quartz.
8. The chip for sample detection of claim 1, wherein the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of a thermoplastic polymer.
9. The chip for sample detection of claim 8, wherein the thermoplastic polymer comprises one or more of polydimethyl methacrylate, polycarbonate, polystyrene, polyamide, and polyethylene terephthalate.
10. A packaging method of a chip for sample detection, comprising:
sealing a gap between an upper end face of a substrate and an upper covering plate; and
sealing a gap between a lower end face of the substrate and a lower covering plate,
wherein the substrate is disposed between the upper covering plate and the lower covering plate, and the substrate is provided with a via hole penetrating the upper end face and the lower end face.
11. The packaging method of the chip for sample detection of claim 10, wherein the sealing a gap between an upper end face of a substrate and an upper covering plate comprises:
binding an adhesive layer and the upper covering plate; and
sealing the gap between the upper covering plate which is bound to the adhesive layer and the upper end face of the substrate.
12. The packaging method of the chip for sample detection of claim 11, wherein the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
13. The packaging method of the chip for sample detection of claim 10, wherein the sealing a gap between a lower end face of the substrate and a lower covering plate comprises:
binding an adhesive layer and the lower covering plate; and
sealing the gap between the lower covering plate which is bound to the adhesive layer and the lower end face of the substrate.
14. The packaging method of the chip for sample detection of claim 13, wherein the adhesive layer is made of a pressure-sensitive double-sided adhesive, a UV-Curing adhesive or an optical grade double-sided adhesive.
15. The packaging method of the chip for sample detection of claim 10, wherein the sealing a gap between an upper end face of a substrate and an upper covering plate comprises:
sealing the gap between the upper end face of the substrate and the upper covering plate directly.
16. The packaging method of the chip for sample detection of claim 10, wherein the sealing a gap between a lower end face of the substrate and a lower covering plate comprises:
sealing the gap between the lower end face of the substrate and the lower covering plate directly.
17. The packaging method of the chip for sample detection of claim 10, wherein the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of one of glass and quartz.
18. The packaging method of the chip for sample detection of claim 10, wherein the upper covering plate and/or the lower covering plate are made of a plate or a film, and are made of a material of a thermoplastic polymer.
19. The packaging method of the chip for sample detection of claim 18, wherein the thermoplastic polymer comprises one or more of polydimethyl methacrylate, polycarbonate, polystyrene, polyamide, and polyethylene terephthalate.
20. The packaging method of the chip for sample detection of claim 10, wherein the chip is a microfluidic chip, and the via hole comprises one or more of a micro channel, a reaction chamber and a detection chamber.
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